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Deep V3 sequencing for HIV type 1 tropism in treatment-naive patients: a reanalysis of the MERIT trial of maraviroc.

机译:初治患者HIV 1型嗜性的深V3测序:对maraviroc的MERIT试验的重新分析。

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BACKGROUND: Deep sequencing is a highly sensitive technique that can detect and quantify the proportion of non-R5 human immunodeficiency virus (HIV) variants, including small minorities, that may emerge and cause virologic failure in patients who receive maraviroc-containing regimens. We retrospectively tested the ability of deep sequencing to predict response to a maraviroc-containing regimen in the Maraviroc versus Efavirenz in Treatment-Naive Patients (MERIT) trial. Results were compared with those obtained using the Enhanced Sensitivity Trofile Assay (ESTA), which is widely used in clinical practice. METHODS: Screening plasma samples from treatment-naive patients who received maraviroc and efavirenz in the MERIT trial were assessed. Samples were extracted, and the V3 region of HIV type 1 glycoprotein 120 was amplified in triplicate and combined in equal quantities before sequencing on a Roche/454 Genome Sequencer-FLX (n = 859). Tropism was inferred from third variable (V3) sequences, with samples classified as non-R5 if >/=2% of the viral population scored
机译:背景:深度测序是一种高度灵敏的技术,可以检测和量化非R5人类免疫缺陷病毒(HIV)变异体(包括少数族裔)的比例,这些变异体可能会在接受含maraviroc方案的患者中出现并引起病毒学衰竭。我们在未接受治疗的患者(MERIT)试验中回顾了深度测序的能力,以预测Maraviroc与Efavirenz对含Maraviroc方案的反应。将结果与使用在临床实践中广泛使用的增强敏感性Trofile分析(ESTA)获得的结果进行比较。方法:评估了在MERIT试验中从接受过maraviroc和efavirenz治疗的未接受过治疗的患者中筛选血浆样品的方法。提取样品,将HIV 1型糖蛋白120的V3区域一式三份扩增,并等量合并,然后在Roche / 454基因组测序仪-FLX上测序(n = 859)。从第三个变量(V3)序列推断出归类,如果使用Geno2pheno将≥2/%的病毒种群评分为

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